In vitro effect of KCA-098, a derivative of coumestrol, on bone resorption of fetal rat femurs

Naoyuki Tsutsumi , Kohtaro Kawashima , Nobuhiko Arai , Hideo Nagata , Masami Kojima , Arao Ujiie , Hiroyoshi Endo
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引用次数: 12

Abstract

The effects of 3,9-bis(N,N-dimethylcarbamoyloxy)-5H-benzofuro[3,2-c]quinoline-6-one (KCA-098), a derivative of coumestrol, on bone resorption was studied in organ cultures of 20-day fetal rat femora. KCA-098 increased the length, dry weight, and calcium and phosphorus contents of parathyroid hormone (PTH)-treated fetal rat femur. As PTH significantly reduced the calcium and phosphorus contents of the femora, probably by stimulating bone resorption, KCA-098 seems to inhibit bone resorption. In fact, KCA-098 inhibited the PTH-induced release of 45Ca from pre-labeled fetal rat femora into the medium in organ culture. Coumestrol also inhibited the release of 45Ca from bone into the medium. However, KCA-098 did not increase the uterine weight of ovariectomized rats, whereas coumestrol did so. Thus KCA-098 is a unique, new inhibitor of bone resorption that has no estrogenic activity.

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库美孕酮衍生物KCA-098对胎鼠股骨骨吸收的体外影响
研究了库美孕酮衍生物3,9-双(N,N-二甲基氨基甲酰氧基)- 5h -苯并呋喃[3,2-c]喹啉-6- 1 (KCA-098)对20日龄胎鼠股骨器官培养骨吸收的影响。KCA-098增加了经甲状旁腺激素(PTH)处理的胎鼠股骨的长度、干重和钙磷含量。由于PTH可能通过刺激骨吸收而显著降低股骨钙磷含量,KCA-098似乎抑制骨吸收。事实上,在器官培养中,KCA-098抑制pth诱导的45Ca从预标记的胎鼠股骨释放到培养基中。库美司醇还能抑制45Ca从骨向培养基的释放。然而,KCA-098并没有增加去卵巢大鼠的子宫重量,而coumestrol却有。因此,KCA-098是一种独特的,新的骨吸收抑制剂,没有雌激素活性。
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Selected bibliography. Socio-economic status and fertility decline: Insights from historical transitions in Europe and North America. Subject index Author index Author index
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